Title: Measles, Mumps and Rubella, an update
1- Measles, Mumps and Rubella, an update
Carol Kerr Consultant Health Protection
Nurse Cheshire Merseyside Health Protection Unit
September 2008
2Measles Epidemiology
- Prior to use of measles vaccine
- Large epidemics every 2nd year with up to 800,000
cases - Mostly pre-school children
- Almost all adults immune to disease
- In 1988 change to MMR
- Coverage 93 - measles now rare
- Unvaccinated children not exposed to natural
infection - Increase in older children and adults
- Often associated with travel and migration
3Diseases not prevalent in UK so do we need to
vaccinate?
- Measles, mumps and rubella now rare due to
success of immunisation programmes - Still killers and causes of disability in
developing countries - Must avoid complacency - recent measles outbreak
in Ireland and clusters in UK
4Measles Disease
- Highly contagious each case will infect 17
people in non immune population - Paramyxovirus
- Respiratory transmission 4 days before to 4 days
after rash onset - High complication rate in malnourished and
immunosuppressed children
5Measles notifications vaccine coverageEngland
and Wales 1950-2000
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6Measles Clinical Features
- Incubation period 10-12 days
- Prodrome
- Fever
- Cough, coryza, conjunctivitis
- Koplik spots
- Rash
- 2-4 days after prodrome, 14 days after exposure
- Maculopapular, becomes confluent
- Begins on face and head
- Persists 5-6 days
7Measles Clinical Features
8Measles Complications
- Diarrhoea 8
- Otitis media and pneumonia 5 10
- Encephalitis 1 in 10,000
- Hospitalisation 1 in 5
- Death 2 in 10,000
9Measles Complications by Age Group
10Mumps Disease
- Moderately contagious viral illness with
respiratory transmission - Paramyxovirus
- Transmission 7 days before to 5 - 9 days after
parotitis onset - Frequent cause of institutional outbreaks in
prevaccine era
11Mumps Clinical Features
- Incubation 14 18 days
- Unspecific prodrome
- Parotitis 30 40
- Up to 20 asymptomatic
- May present as lower respiratory illness,
particularly in preschool children
12Parotitis
13Mumps Complications
- Meningitis 20 usually benign
- Orchitis 20 in postpubertal males
- Pancreatitis 2 5
- Deafness 1 in 20,000
- Death very rare
14Mumps in a Healthcare Setting
- Nosocomial transmission rare
- No evidence complication rate higher in
immunosuppressed - Isolate patient or exclude staff for 9 days after
onset of symptoms - Respiratory precautions (gown and gloves)
- Do not exclude staff contacts from work
- Re-deploy non immune contacts with symptoms if
working in high risk setting (from day 12 to 25
after exposure)
15Mumps - Cheshire Merseyside 2005
16Mumps Laboratory Diagnosis
- Isolation of mumps virus
- Serology
- positive IgM antibody or significant increase in
IgG - Saliva positive IgM
17Mumps in Pregnancy
- Reassure
- Evidence for increased risk of foetal loss in 1st
trimester weak - No evidence increased risk severe congenital
abnormality - Do not exclude pregnant women from setting such
as work during mumps outbreak
18Mumps and Measles Control and Prevention
- MMR
- Routine childhood immunization age 12-15 months
and preschool - Catch up campaign for students and school leavers
- Check vaccination status at school entry
- Check immunity of health care workers and
international travelers history of disease or 2
MMR - Breastfeeding
- Reduce poverty
19Response to a Case
- On call action usually none
- Notify to Health Protection Agency
- Exclude from school or work for 5 days from
symptom onset - Check vaccination status
- Laboratory confirmation usually saliva test
- Post-exposure vaccination will not prevent
infection
20Epidemiology of rubella
- Last outbreak occurred in 1996
- Most cases young adult males
- Not vaccinated routinely with MMR
- Too old for MR campaign in 1994
- Rubella infection now exceedingly rare in UK
- Congenital rubella syndrome now rare
- Small increase in CRS associated with 1996
outbreak - Small number of antenatal women are still at risk
- Protection from exposure
21Risk of intrauterine transmission during
different stages of pregnancy
22Rubella clinical feature
23Rubella (German Measles)
- For most people rubella is a mild infectious
disease, although it can have serious
consequences for pregnant women. It was
previously common among children aged four to
nine years. - It is transmitted by direct contact or droplet
spread. Humans are the only known hosts.
24Clinical presentation
- It causes a transient red rash, swollen lymph
glands around the ears (post-auricular) and back
of head (sub-occipital), and occasionally in
adults, arthritis (any abnormality of a joint
caused by inflammation) and arthralgia (pain in a
joint caused by inflammation). - The rash may be fleeting and may look like the
rash caused by other viruses, therefore, clinical
diagnosis by rash is unreliable - The incubation period is 14 - 21 days
25Rubella
- Clinical diagnosis is unreliable as the rash may
be fleeting and is not specific to rubella. - Rubella is spread by droplet transmission.
- The incubation period is 14 to 21days, with the
majority of individuals developing a rash 14 to
17 days after exposure. - Individuals with rubella are infectious from one
week before symptoms
26Can MMR cause autism?
- Wakefield et al 1998 Lancet - suggested link
between MMR and new syndrome - Parental testimonies of regressive autism after
MMR - Wakefield et al 1999 Lancet - suggested rise in
autism in UK California coincided with
introduction of MMR
27Can MMR cause autism?
- Wakefields 1998 work rejected by scientific
community - flawed methodology, only 12 subjects,
biologically implausible - Taylor et al 1999 Lancet - N.Thames study of 498
cases autism - no clustering of onsets shortly after MMR
- no age difference at diagnosis for vaccinated or
unvaccinated at 18 months
28Vaccine safety testing
- Trials carried out in 3 phases
- I - small number healthy adult volunteers
- II - sample 100-200 of intended recipients
- III - protection against disease evaluated by
comparing vaccinated and unvaccinated - Prior to general use, each batch has extensive
quality control and safety testing - Extensive post-marketing surveillance
29Vaccine licensing
- Tens of millions of doses MMR given before
introduction in UK and shown to be safe and
highly effective - Ongoing surveillance for adverse events via
case-note tagging and yellow card system
30Why two doses of MMR?If uptake is 88, 12
unvaccinated and without a second dose
- 10 dont respond to measles component
- So 21 of children susceptible to measles in one
school year - Enough to risk large outbreak every 4-5 years
- Herd immunity needs to be 95 (i.e. only 5
susceptible) to eliminate spread
- 13 dont respond to mumps component
- So 25 susceptible to mumps in one school year
- Potential for continuing outbreaks, especially in
school age children (42 of confirmed cases in
10-14 yr olds had received a single dose)
31Why a second dose (contd)
- 90 of children who failed to respond to single
dose of MMR, respond to second dose - So
- second dose produces a response in most children
who failed to respond to first dose, thus
reducing number of those susceptible - is an opportunity to immunise those who have not
had any doses - acts as booster for those who were protected
first time around
32Summary
- Control of measles and rubella good
- Increase in measles in 2002in line with
predictions - size of outbreaks similar to those previously
described - national increase in notifications (? due to
increased awareness) - Increase in mumps since 1998 in older school age
children e.g. Bootle outbreak - MMR coverage has dropped (83 nationally, below
80 in Sefton) - 2 doses necessary to prevent resurgences and give
long term protection to individual children
33and finally
- Thank you.
- Any questions?
- www.hpa.org.uk Carol.kerr_at_hpa.org.uk 0151
290 8360